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Current Neuropharmacology
ISSN: 1570-159X
Current Neuropharmacology
Volume 3, Number 2, April 2005
Contents
Developing Pharmacotherapies for Cannabis and Cocaine Use
Disorders Pp. 95-114
Carl L. Hart and Wendy J. Lynch
[Abstract]
Sensory-Motor Integration in the Medial Medulla Pp.
115-143
Yuan-Yang Lai and Jerome M. Siegel
[Abstract]
Pharmacology of Motor and Somatosensory Skills in Humans
Pp. 145-156
Burkhard Pleger, Martin Tegenthoff, Hubert Dinse,
Patrick Ragert and Peter Schwenkreis
[Abstract]
Regional Differences in Adaptation of CNS Mu Opioid Receptors
to Chronic Opioid Agonist Administration Pp. 157-182
L.J. Sim-Selley
[Abstract]
Hypoxia as an Initiator of Neuroinflammation: Microglial
Connections Pp. 183-191
Jiyeon Ock, Hee-Jung Cho, Su Hyung Hong, In Kyeom Kim and
Kyoungho Suk
[Abstract]
Abstracts
[Back to top]
Developing Pharmacotherapies for Cannabis and Cocaine Use
Disorders
Carl L. Hart and Wendy J. Lynch
Despite the fact that more people seek treatment for cannabis-related
disorders than for any other illicit substance-related disorder
in the U.S., there are no medications approved for the treatment
of these disorders. Similarly, more than half of those meeting
criteria for a cocaine use disorder seek treatment. Yet, after
two decades of intense medications development research efforts,
there remains no approved cocaine pharmacotherapy. This paper
reviews data from recent research investigations that may
be relevant for the development of pharmacotherapies for cannabis-
and cocaine-related disorders. Included in the discussion
are findings from studies that have assessed the ability of
medications to ameliorate cannabis- and cocaine-related abstinence
symptoms in laboratory animals and human research participants.
Data from studies that have investigated the effects of pharmacological
agents on response to cannabis and cocaine are also reviewed
because these data may provide information critical for informing
relapse prevention medication development efforts. The majority
of published studies evaluating cannabis pharmacotherapies
have focused on decreasing withdrawal symptoms: a growing
number of medications reduce symptoms in laboratory animals,
but the majority of these findings have not been replicated
in humans. Fewer studies have assessed the effects of potential
cannabis treatment medications on cannabinoid-related reinforcing
effects. In laboratory animals, only one has shown promise,
while in humans, no medication has been demonstrated to alter
marijuana self-administration behavior. Numerous medications
have been examined for treating cocaine use disorders; in
general, none have proven effective. Some medications, however,
have demonstrated utility within subpopulations of cocaine-dependent
individuals, suggesting that like psychosocial treatment,
pharmacotherapy may need to be tailored to the individual.
[Back to top]
Sensory-Motor Integration in the Medial Medulla
Yuan-Yang Lai and Jerome M. Siegel
The rostromedial medulla, including the nucleus gigantocellularis
(NGC) and magnocellularis (NMC), plays a role as a relay nucleus
for both the sensory and motor systems. The NGC/NMC is important
in the modulation of somatic and visceral activities. Electrophysiological
and pharmacological studies have shown that the NGC/NMC is
involved in nociception, locomotion, regulation of basal muscle
tone, sleep, as well as cardiovascular and pulmonary activities.
Pharmacological and electrical stimulation of the NGC/NMC
can produce opposite effects on physiological functions: analgesia
or hyperalgesia, and suppression or facilitation of motor
activity, depending on the subgroups of neurons activated
and the states of the sleep-wake cycle at the time of stimulation.
Sensory inputs including noxious and innocuous stimuli converge
on the NGC/NMC. The NGC/NMC also plays a role as a relay nucleus,
which sends sensory information to the higher centers. The
NGC/NMC receives projections from the supra-bulbar motor facilitatory
and inhibitory areas, and plays an important role in the regulation
of motor activity. Pharmacologically, neurons in the NGC/NMC
contribute to opioid, glutamate, GABA, acetylcholine, dopamine,
substance P, neurotensin, hypocretin (orexin), and cannabinoid
mediated sensory and motor activities, as well as cardiovascular
and pulmonary functions. In this review, we will discuss the
neuronal morphology, physiological functions and pharmacological
characterization of the rostromedial medulla. We will consider
the evidence that dysfunction of the NGC/NMC is a factor in
a number of neurological diseases, including Parkinson’s
disease, restless legs syndrome, periodic leg movement, REM
sleep behavior disorder, amyotrophic lateral sclerosis and
narcolepsy.
[Back to top]
Pharmacology of Motor and Somatosensory Skills in Humans
Burkhard Pleger, Martin Tegenthoff, Hubert Dinse, Patrick
Ragert and Peter Schwenkreis
The pharmacological basis of changes in human behaviour
and associated cortical reorganization remains poorly understood.
Different paradigms have been introduced to alter motor and
somatosensory skills in humans. The underlying changes in
synaptic efficacy can be modulated by pharmacological agents
acting to gate synaptic plasticity. Non-invasive imaging techniques
offer the possibility to assess parallel changes in cortical
processing.
Cellular studies suggest that there might be only few, but
very basic mechanisms that control regulation of synaptic
transmission. In particular, the γ-aminobutyric
acid (GABA) and the N-methyl-D-aspartic acid (NMDA) receptor,
a specific subtype of the glutamatergic receptors, are thought
to be crucial in synaptic plasticity. Thus, the application
of benzodiazepines facilitating the binding of GABA on GABA(A)
receptors, and NMDA receptor blockers, were found to prevent
learning and associated cortical reorganization.
While there are many approaches to block plastic processes,
less is known about drugs, which enhance learning and cortical
plasticity. Growing evidence from human studies support the
suggestion that learning is subject to amplification by amphetamine.
Amphetamine however acts non-specific by increasing centrally
the levels of dopamine, serotonin, and noradrenaline. Thus,
first approaches that intend to scrutinize the apparently
ubiquitous role of only one of these neurotransmitter systems
used more specifically acting pharmacological agents.
In this review we focus on studies that aimed to investigate
the pharmacology of the motor and somatosensory system. First,
we introduce standards for testing potential effects of a
substance. Then, we focus on biochemical mechanisms of learning,
before discussing different motor and somatosensory paradigms
which were introduced to elicit changes in cortical excitability
or organization in animals and humans. Emphasis is placed
on the role of inhibitory and excitatory pharmacological agents
acting to gate synaptic plasticity in healthy subjects and
patients. It is concluded that future studies that investigate
the interaction between artificially modulated receptor activity
and specific patterns of behaviour in various neurological
disorders may help to improve our understanding of how to
support recovery of motor and somatosensory function pharmacologically.
[Back to top]
Regional Differences in Adaptation of CNS Mu Opioid Receptors
to Chronic Opioid Agonist Administration
L.J. Sim-Selley
Opioids produce a number of acute effects, notably antinociception
and euphoria, whereas chronic use produces tolerance and dependence.
Mu opioid receptors (MOR) mediate opioid antinociception and
reinforcement and are distributed throughout the CNS in regions
consistent with their acute effects, including striatum, thalamus,
amygdala, periaqueductal gray (PAG), locus coeruleus (LC),
and spinal cord. G-protein-coupled receptor (GPCR) adaptation
involves G-protein-coupled receptor kinase (GRK)-mediated
receptor phosphorylation with subsequent β-arrestin
binding, which uncouples GPCRs from G-protein activation.
β-arrestin
binding can initiate receptor endocytosis, leading to subsequent
degradation or recycling of GPCRs. These processes are reflected
experimentally by desensitization (loss of functional response)
and downregulation (loss of receptor binding sites). Evaluation
of MOR levels following chronic opioid treatment has indicated
that MOR downregulation is not required for the expression
of tolerance and dependence. In contrast, evaluation of post-receptor
events has revealed region-dependent alterations in MOR-G-protein
coupling and subsequent effector activity. For example, MOR-mediated
G-protein activity and inhibition of adenylyl cyclase are
generally decreased in brainstem nuclei following chronic
morphine administration, whereas no changes are found in striatum.
Similarly, tolerance develops to MOR-mediated potassium channel
activation in regions that include LC and PAG. Chronic opioid-mediated
effects on adenylyl cyclase affect downstream signaling via
regulation of cAMP dependent protein kinase (PKA) and cAMP
response element binding protein (CREB), both of which are
altered in LC, nucleus accumbens (NAC) and amygdala, regions
that might contribute to motivational and physiological signs
of withdrawal. Possible explanations for regional differences
in MOR adaptation include region-specific co-localization
of MOR with signaling proteins and differential distribution
of MOR splice variants or oligomers. Moreover, the finding
that regional differences exist in neuroadaptation suggests
that behavioral adaptations to chronic opioid administration
will vary based on the functional neuroanatomy of the MOR
system.
[Back to top]
Hypoxia as an Initiator of Neuroinflammation: Microglial
Connections
Jiyeon Ock, Hee-Jung Cho, Su Hyung Hong, In Kyeom Kim and
Kyoungho Suk
Hypoxia, which is a lowered physiological oxygen tension,
is an important biological signal as well as a component of
many diseases. In central nervous system, hypoxia is associated
with brain injury following the ischemic stroke. Recent studies
indicate that hypoxia may not only induce a direct neuronal
damage, but it may also initiate inflammatory responses by
activating microglia. Toxic inflammatory mediators produced
by activated microglia under hypoxic conditions exacerbate
the neuronal injury during cerebral ischemia. Pharmacological
inhibition of hypoxic activation of microglia may prove to
be neuroprotective against ischemic stroke.
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